npj Vaccines (May 2022)

Adjuvanting a subunit SARS-CoV-2 vaccine with clinically relevant adjuvants induces durable protection in mice

  • Lilit Grigoryan,
  • Audrey Lee,
  • Alexandra C. Walls,
  • Lilin Lai,
  • Benjamin Franco,
  • Prabhu S. Arunachalam,
  • Yupeng Feng,
  • Wei Luo,
  • Abigail Vanderheiden,
  • Katharine Floyd,
  • Samuel Wrenn,
  • Deleah Pettie,
  • Marcos C. Miranda,
  • Elizabeth Kepl,
  • Rashmi Ravichandran,
  • Claire Sydeman,
  • Natalie Brunette,
  • Michael Murphy,
  • Brooke Fiala,
  • Lauren Carter,
  • Robert L. Coffman,
  • David Novack,
  • Harry Kleanthous,
  • Derek T. O’Hagan,
  • Robbert van der Most,
  • Jason S. McLellan,
  • Mehul Suthar,
  • David Veesler,
  • Neil P. King,
  • Bali Pulendran

DOI
https://doi.org/10.1038/s41541-022-00472-2
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 14

Abstract

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Abstract Adjuvants enhance the magnitude and the durability of the immune response to vaccines. However, there is a paucity of comparative studies on the nature of the immune responses stimulated by leading adjuvant candidates. In this study, we compared five clinically relevant adjuvants in mice—alum, AS03 (a squalene-based adjuvant supplemented with α-tocopherol), AS37 (a TLR7 ligand emulsified in alum), CpG1018 (a TLR9 ligand emulsified in alum), O/W 1849101 (a squalene-based adjuvant)—for their capacity to stimulate immune responses when combined with a subunit vaccine under clinical development. We found that all four of the adjuvant candidates surpassed alum with respect to their capacity to induce enhanced and durable antigen-specific antibody responses. The TLR-agonist-based adjuvants CpG1018 (TLR9) and AS37 (TLR7) induced Th1-skewed CD4+ T cell responses, while alum, O/W, and AS03 induced a balanced Th1/Th2 response. Consistent with this, adjuvants induced distinct patterns of early innate responses. Finally, vaccines adjuvanted with AS03, AS37, and CpG1018/alum-induced durable neutralizing-antibody responses and significant protection against the B.1.351 variant 7 months following immunization. These results, together with our recent results from an identical study in non-human primates (NHPs), provide a comparative benchmarking of five clinically relevant vaccine adjuvants for their capacity to stimulate immunity to a subunit vaccine, demonstrating the capacity of adjuvanted SARS-CoV-2 subunit vaccines to provide durable protection against the B.1.351 variant. Furthermore, these results reveal differences between the widely-used C57BL/6 mouse strain and NHP animal models, highlighting the importance of species selection for future vaccine and adjuvant studies.